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诊断止血实验室对因子抑制剂的错误识别:认识陷阱并阐明策略。大型多中心评估的后续研究。

Mis-identification of factor inhibitors by diagnostic haemostasis laboratories: recognition of pitfalls and elucidation of strategies. A follow up to a large multicentre evaluation.

作者信息

Favaloro Emmanuel J, Bonar Roslyn, Duncan Elizabeth, Earl Gail, Low Joyce, Aboud Margaret, Just Sarah, Sioufi John, Street Alison, Marsden Katherine

机构信息

Department of Haematology and Royal College of Pathologists of Australasia Quality Assurance Program, Institute of Clinical Pathology and Medical Research, Westmead Hospital, New South Wales 2145, Australia.

出版信息

Pathology. 2007 Oct;39(5):504-11. doi: 10.1080/00313020701569998.

Abstract

AIMS

We previously reported the ability of diagnostic haemostasis facilities to identify coagulation factor abnormalities and inhibitors, through a large multi-centre study conducted on behalf of the Royal College of Pathologists of Australasia (RCPA) Quality Assurance Program (QAP). In the current report, additional data evaluation aims to (1) help identify the reasons behind the failures in inhibitor identification, (2) highlight the pitfalls in inhibitor testing, and (3) help elucidate some strategies for overcoming these problems and to assist in better identification and characterisation of inhibitors.

METHODS

Forty-two laboratories blind tested a set of eight samples for the presence or absence of inhibitors. These included true factor inhibitors (FVIII and FV), and other samples that reflected potential pre-analytical variables (e.g., heparin contamination, serum, EDTA plasma, aged plasma) that might arise and complicate inhibitor detection or lead to false inhibitor identification.

RESULTS

There was a wide scatter of inhibitor results, with false positive and false negative inhibitor identification, and mis-identification of inhibitors (e.g., FVIII inhibitor identified where FV inhibitor present). Further analysis of the pattern of reported laboratory results, including routine coagulation testing and factor profiles, allowed some additional interpretative power to provide strategies that will assist laboratories to improve the accuracy of inhibitor identification in the future.

CONCLUSIONS

There are currently occasional lapses in factor inhibitor identification, which this report will hopefully help address.

摘要

目的

我们之前通过代表澳大利亚皇家病理学家学院(RCPA)质量保证计划(QAP)开展的一项大型多中心研究,报告了诊断止血设施识别凝血因子异常和抑制剂的能力。在本报告中,额外的数据评估旨在:(1)帮助确定抑制剂识别失败背后的原因;(2)突出抑制剂检测中的陷阱;(3)帮助阐明克服这些问题的一些策略,并协助更好地识别和表征抑制剂。

方法

42个实验室对一组8个样本进行了抑制剂存在与否的盲测。这些样本包括真正的因子抑制剂(FVIII和FV),以及其他反映可能出现并使抑制剂检测复杂化或导致抑制剂错误识别的潜在分析前变量的样本(如肝素污染、血清、EDTA血浆、老化血浆)。

结果

抑制剂检测结果差异很大,存在抑制剂的假阳性和假阴性识别以及抑制剂的错误识别(如存在FV抑制剂时却识别为FVIII抑制剂)。对报告的实验室结果模式(包括常规凝血检测和因子谱)进行进一步分析,能提供一些额外的解释力,从而制定有助于实验室提高未来抑制剂识别准确性的策略。

结论

目前在因子抑制剂识别方面偶尔会出现失误,希望本报告能有助于解决这一问题。

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